Scientific Reports (Oct 2023)

Design of hypoxia responsive CRISPR-Cas9 for target gene regulation

  • Yan An,
  • Chandana S. Talwar,
  • Kwang-Hyun Park,
  • Woo-Chan Ahn,
  • Su-Jin Lee,
  • Seong-Ryeong Go,
  • Jin Hwa Cho,
  • Do Yon Kim,
  • Yong-Sam Kim,
  • Sayeon Cho,
  • Jeong-Hoon Kim,
  • Tae-Jip Kim,
  • Eui-Jeon Woo

DOI
https://doi.org/10.1038/s41598-023-43711-9
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 14

Abstract

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Abstract The CRISPR–Cas9 system is a widely used gene-editing tool, offering unprecedented opportunities for treating various diseases. Controlling Cas9/dCas9 activity at specific location and time to avoid undesirable effects is very important. Here, we report a conditionally active CRISPR–Cas9 system that regulates target gene expression upon sensing cellular environmental change. We conjugated the oxygen-sensing transcription activation domain (TAD) of hypoxia-inducing factor (HIF-1α) with the Cas9/dCas9 protein. The Cas9-TAD conjugate significantly increased endogenous target gene cleavage under hypoxic conditions compared with that under normoxic conditions, whereas the dCas9-TAD conjugate upregulated endogenous gene transcription. Furthermore, the conjugate system effectively downregulated the expression of SNAIL, an essential gene in cancer metastasis, and upregulated the expression of the tumour-related genes HNF4 and NEUROD1 under hypoxic conditions. Since hypoxia is closely associated with cancer, the hypoxia-dependent Cas9/dCas9 system is a novel addition to the molecular tool kit that functions in response to cellular signals and has potential application for gene therapeutics.